Single-cell transcriptomics and epigenomics unravel the role of monocytes in neuroblastoma bone marrow metastasis.
Irfete S FetahuWolfgang Esser-SkalaRohit DnyansagarSamuel SindelarFirkret RifatbegovicAndrea BileckLukas SkosEva BozsakyDaria LazicLisa Ellen ShawMarcus TötzlDora TarlungeanuMarie BernkopfMagdalena RadosWolfgang WeningerEleni M TomazouChristoph BockChristopher GernerRuth Lydia LadensteinMatthias FarlikNikolaus FortelnySabine Taschner-MandlPublished in: Nature communications (2023)
Metastasis is the major cause of cancer-related deaths. Neuroblastoma (NB), a childhood tumor has been molecularly defined at the primary cancer site, however, the bone marrow (BM) as the metastatic niche of NB is poorly characterized. Here we perform single-cell transcriptomic and epigenomic profiling of BM aspirates from 11 subjects spanning three major NB subtypes and compare these to five age-matched and metastasis-free BM, followed by in-depth single cell analyses of tissue diversity and cell-cell interactions, as well as functional validation. We show that cellular plasticity of NB tumor cells is conserved upon metastasis and tumor cell type composition is NB subtype-dependent. NB cells signal to the BM microenvironment, rewiring via macrophage mgration inhibitory factor and midkine signaling specifically monocytes, which exhibit M1 and M2 features, are marked by activation of pro- and anti-inflammatory programs, and express tumor-promoting factors, reminiscent of tumor-associated macrophages. The interactions and pathways characterized in our study provide the basis for therapeutic approaches that target tumor-to-microenvironment interactions.